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Am J Physiol Regul Integr Comp Physiol 280: R1-R7, 2001;
0363-6119/01 $5.00
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Vol. 280, Issue 1, R1-R7, January 2001

Endothelin and nitric oxide mediate reduced myogenic reactivity of small renal arteries from pregnant rats

Robin E. Gandley1, Kirk P. Conrad1,2, and Margaret K. McLaughlin1,2

Departments of 1 Obstetrics, Gynecology and Reproductive Sciences, and 2 Cell Biology and Physiology, University of Pittsburgh and Magee-Womens Research Institute, Pittsburgh, Pennsylvania 15213

We tested the hypothesis that endothelin acting through the endothelial ETB receptor subtype and the nitric oxide (NO) pathway accounts for reduced myogenic reactivity of the renal resistance vasculature during pregnancy. Small renal arteries (100-200 µm) were isolated from virgin and midterm pregnant rats when gestational renal hyperfiltration and vasodilation are maximal in this species. Myogenic reactivity (the adjustment of arterial diameter in response to a change in transmural pressure) was assessed with a pressurized myograph system. A rapid increase in transmural pressure from 60 to 80 mmHg resulted in a 2.4% diameter increase in vessels from virgin compared with an 8.1% increase in arteries from midgestation rats (n = 8 each, P < 0.05). Thus myogenic reactivity is markedly reduced during pregnancy. Incubation with the NO synthase inhibitors, an ETB receptor subtype antagonist (RES-701-1), the nonselective ETA/B receptor blocker (SB-209670), or endothelial removal abrogated the reduced myogenic reactivity of vessels from gravid rats without affecting myogenic reactivity in arteries from virgin animals. Thus the endothelium mediates the reduced myogenic reactivity of small renal arteries of midgestation rats most likely through the ETB receptor subtype and NO pathway.

resistance vasculature; NG-monomethyl-L-arginine; endothelin receptors; RES-701-1; renal circulation


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